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两性霉素 B 载固体脂质纳米粒(SLNs)和纳米结构脂质载体(NLCs):载药量和药物生物利用度特性的影响。

Amphotericin B-loaded solid lipid nanoparticles (SLNs) and nanostructured lipid carrier (NLCs): effect of drug loading and biopharmaceutical characterizations.

机构信息

a Faculty of Pharmaceutical Sciences , Chulalongkorn University , Bangkok, Thailand.

b Faculty of Pharmaceutical Sciences , Prince of Songkla University , Songkhla, Hat-Yai, Songkhla , Thailand.

出版信息

Drug Dev Ind Pharm. 2018 Oct;44(10):1693-1700. doi: 10.1080/03639045.2018.1492606. Epub 2018 Jul 23.

Abstract

The aim of this study was to further investigate the effect of drug loading, drug entrapment efficiency, the drug release profiles and biopharmaceutical point of views of amphotericin B (AmB) lipid formulations, that is, degree of aggregation by UV-spectroscopy, in vitro hemolytic and antifungal activities. The optimum drug loading was 2.5% by weight corresponded to lipid fraction in formulation. Increasing of the drug entrapment was achieved by blending small amount of phospholipid in solid lipid nanoparticle (SLN) dispersions. All AmB lipid dispersions were less aggregated species and hemolytic response than Fungizone indicating that lipid nanoparticles could reduce its toxicity. The sustained release profiles of AmB formulations depended on its aggregated form and entrapment efficiency. Too high AmB loaded (5% w/w) showed a biphasic drug release profile probably due to some amounts of drug deposited on the nanosphere surface including in continuous phase which promptly released. For in vitro antifungal testing, all AmB lipid formulations were equal and more effective than both AmB itself and Fungizone. These observations suggested that AmB loaded SLNs, nanostructured lipid carriers and modified SLNs by blending lecithin could enhance AmB solubility, prolong release characteristics, reduce toxicity and improve antifungal activity.

摘要

本研究旨在进一步探讨两性霉素 B(AmB)脂质制剂的载药量、药物包封效率、药物释放特性和生物药剂学特性,即通过紫外光谱法研究其聚集程度、体外溶血活性和抗真菌活性。最佳载药量为 2.5%(重量比),对应于制剂中的脂质部分。通过在固体脂质纳米粒(SLN)分散体中混合少量磷脂,可以提高药物包封率。所有 AmB 脂质分散体的聚集程度和溶血反应均低于 Fungizone,表明脂质纳米粒可以降低其毒性。AmB 制剂的持续释放特性取决于其聚集形式和包封效率。过高的 AmB 载药量(5%w/w)显示出双相药物释放曲线,可能是由于纳米球表面包括连续相中有一些药物沉积,这些药物迅速释放。对于体外抗真菌测试,所有 AmB 脂质制剂与 AmB 本身和 Fungizone 相比,效果相等且更有效。这些观察结果表明,负载 AmB 的 SLN、纳米结构脂质载体和通过混合卵磷脂改性的 SLN 可以提高 AmB 的溶解度、延长释放特性、降低毒性和提高抗真菌活性。

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